S254

ESTRO 35 2016

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OC-0540

IOERT after gross total resection combined with EBRT in

extremity sarcoma: a pooled analysis

F. Roeder

1

German Cancer Research Center DKFZ, Molecular Radiation

Oncology, Heidelberg, Germany

1,2

, A. De Paoli

3

, I. Alldinger

4

, G. Bertola

3

, G. Boz

3

,

J. Garcia-Sabrido

5

, M. Uhl

6

, A. Alvarez

7

, B. Lehner

8

, F. Calvo

7

,

R. Krempien

9

2

University Hospital of Munich LMU, Radiation Oncology,

Munich, Germany

3

National Cancer Institute, Radiation Oncology, Aviano, Italy

4

University of Heidelberg, Surgery, Heidelberg, Germany

5

University Hospital Gregorio Maranon, Surgery, Madrid,

Spain

6

University of Heidelberg, Radiation Oncology, Heidelberg,

Germany

7

University Hospital Gregorio Maranon, Radiation Oncology,

Madrid, Spain

8

University of Heidelberg, Orthopedics, Heidelberg, Germany

9

Helios Clinic, Radiation Oncology, Berlin, Germany

Purpose or Objective:

In 2009 we reported promising first

results of a European pooled analysis which evaluated the use

of intraoperative radiation therapy (IORT) in the treatment of

soft tissue sarcomas. However, comparison of these results

with non-IORT series seemed difficult, mainly because of the

inclusion of grossly incomplete resected lesions, patients

treated without additional external beam radiation therapy

(EBRT) and comparatively short follow-up. Therefore we re-

analyzed our data limited to the patients who received IOERT

preceeded or followed by EBRT after gross total resection

with extended follow-up.

Material and Methods:

Three European expert centers

participated in the current analysis. Patients with gross

incomplete resection, missing documentation of EBRT or

primary lesions outside the extremities were excluded,

leaving 259 patients for analysis. Median age was 55 years

and median tumor size 8 cm. 80% of the patients presented in

primary situation with 81% of the tumors located in the lower

limb. Stage at presentation was I:9%, II:47%, III:39%, IV:5%.

Most patients showed high grade lesions (FNCLCC grade 1:9%,

2:34%, 3:58%, predominantly liposarcoma (31%) and MFH

(27%). IOERT was applied to the tumor bed with a median

dose of 12 Gy using a median electron energy of 8 MeV.

IOERT was preceeded (17%) or followed (83%) by EBRT with a

median dose of 45 Gy in all patients. 37% of the patients

received additional chemotherapy.

Results:

Median follow up was 63 months. Surgery resulted in

free margins (R0) in 71% while 29% suffered from microscopic

positive margins (R1). We observed 27 local failures,

transferring into a 5-year local control rate of 86%. Univariate

analysis revealed primary vs recurrent situation and resection

margin as significant factors for local control but only

resection margin (5-year LC rate 94% vs 70%, HR 3.8)

remained significant in multivariate analysis. Distant failure

was found in 70 patients, resulting in a 5-year distant control

rate of 69%. Factors with significant impact on distant control

in univariate analysis were histology, grading, resection

margin and stage IV prior/at IOERT, but only grading and

stage IV remained significant in multivariate analysis.

Actuarial 5-year rates of FFTF and OS were 61% and 78%,

respectively. Significant factors for overall survival were only

grading and stage IV prior/at IOERT (uni- and multivariate).

Secondary amputations were needed in 14 patients (5%)

resulting in a final limb-preservation rate of 95%. Good

functional outcome was achieved in 81%.

Conclusion:

Combination of IOERT and EBRT after limb

sparing surgery resulted in encouraging local control and

overall survival with excellent rates of preserved limb

function in this unfavourable patient group. Our analysis

identified resection margin as most important factor for local

control while overall survival was mainly influenced by

grading and stage IV prior/at IOERT.

OC-0541

Long-term results of the AIEOP MH-89 protocol for

pediatric Hodgkin lymphoma

M. Robazza

1

CRO - Aviano Cancer Center, Pediatric Radiotherapy Unit,

Aviano, Italy

1

, M. Mascarin

1

, C. Elia

1

, A. Todesco

2

, G.

Scarzello

3

, A. Pession

4

, A. Garaventa

5

, S. Barra

6

, M. Zecca

7

,

N. Santoro

8

, M. Bianchi

9

, U. Riccardi

10

, F. Locatelli

11

, R. De

Santis

12

, P. Indolfi

13

, M. Nardi

14

, F. Porta

15

, T. Casini

16

, C.

Consarino

17

, S. D’Amico

18

, M. Provenzi

19

, G.A. Zanazzo

20

, P.

Farruggia

21

, G. Guerrini

22

, R. Burnelli

22

2

Azienda Ospedaliera -Universita’ di Padova, Clinica di

Oncoematologia Pediatrica, Padova, Italy

3

Azienda Ospedaliera -Universita’ di Padova, U.O. di

Radioterapia, Padova, Italy

4

Clinica Pediatrica-Policlinico Sant’Orsola Malpighi, U.O. di

Oncologia ed Ematologia “Lalla Seràgnoli”, Bologna, Italy

5

Ospedale Gaslini, U.O. di Ematooncologia Pediatrica,

Genova, Italy

6

Istituto Tumori Genova, U.O. di Radioterapia, Genova, Italy

7

Policlinico San Matteo, U.O. di Oncoematologia pediatrica,

Pavia, Italy

8

Policlinico di Bari, U.O. di Oncoematologia Pediatrica, Bari,

Italy

9

Ospedale Regina Margherita, U.O. di Oncoematologia

Pediatrica, Torino, Italy

10

Ospedale le Molinette, U.O. di Radioterapia, Torino, Italy

11

Ospedale Bambin Gesù, U.O. di Ematoncologia Pediatrica,

Roma, Italy

12

Casa Sollievo della Sofferenza, U.O. di Oncologia

Pediatrica, San Giovanni Rotondo, Italy

13

Università Federico II- policlinico di Napoli, U.O. di

Ematooncologia Pediatrica, Napoli, Italy

14

Azienda Ospedaliera - Universita' Pisana Ospedale S.

Chiara, U.O. di Oncoematologia Pediatrica, Pisa, Italy

15

Ospedale dei Bambini, U.O. di Oncoematologia Pediatrica,

Brescia, Italy

16

Azienda Ospedaliero-Universitaria Meyer, Dipartimento A.I.

Oncoematologia SODC Tumori pediatrici e Trapianto di

cellule staminali, Firenze, Italy

17

Azienda Ospedaliero Pugliese-Ciaccio, U.O. di Oncologia

Pediatrica, Catanzaro, Italy

18

Clinica Pediatrica, U.O. di Oncologia Pediatrica, Catania,

Italy

19

Ospedali Riuniti, U.O. di Onco Ematologia Pediatrica,

Bergamo, Italy

20

Università degli studi di Trieste Ospedale Infantile Burlo

Garofolo, U.O. Emato-Oncologia Pediatrica, Trieste, Italy

21

A.R.N.A.S. Civico di Cristina e Benfratelli, U.O.

Oncoematologia Pediatrica, Palermo, Italy

22

Azienda Ospedaliero-Universitaria di Ferrara S.Anna, U.O.

di Oncoematologia Pediatrica, Ferrara, Italy

Purpose or Objective:

The AIEOP-MH89 protocol aimed to

optimize treatment results in pediatric Hodgkin lymphoma

compared to the previous AIEOP-MH83 protocol. Modifications

included: involved field instead of extended field radiation

therapy (RT) in early-stage patients (pts); anticipated RT for

pts with a mass/thorax ratio (M/T)>0.33; enrolment of

advanced-stage pts in SIOP HD IV protocol.

Material and Methods:

Between 1989-1995, 254 evaluable

pts (median age 10 years, range 2-15 years) received the

AIEOP-MH89 protocol. The pts were divided into 3

chemotherapeutic groups according to the clinical stage.

Group (GR) 1, pts in stages IA and IIA, including those with a

mass/thorax ratio (M/T)<0.33, received 3 cycles of

adriamycin, bleomycin, vinblastine, and imidazole

carboxamide (ABVD). RT was given after completion of

chemotherapy. GR 2, pts in stages IEA, IB, IA, IIA with

M/T>0.33, IIB, IIEB, IIIA, IIIS, and IIEA, was treated with

alternating cycles of nitrogen mustard, vincristine,

procarbazine, and prednisone (MOPP)/ABVD. The therapeutic

program included 2 cycles of MOPP/ABVD before radiation

therapy and 4 cycles MOPP/ABVD after RT. GR 3, pts in

advanced stages IIIB, IVA and IVB, was treated according to

the SIOP HD IV-87 protocol, with 2 cycles of vincristine,

procarbazine, prednisone, adriamycin, (OPPA) and 2 cycles of